Do post-translational beta cell protein modifications trigger type 1 diabetes?

Størling, Joachim; Overgaard, Jesper; Brorsson, Caroline; Piva, Francesco; Bang-Berthelsen, Claus Heiner; Haase, Claus; Nerup, Jørn; Pociot, Flemming

doi:10.1007/s00125-013-3045-3

Cited by 18 publications

(21 citation statements)

References 66 publications

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“…High levels of ROS may lead to oxidative post-translational modification (oxPTM) of beta cell self-proteins and the formation of neoepitopes. Neoepitopes are epitopes that have not been previously presented to the immune system [3,4] and therefore escape immune tolerance and generate autoimmunity. Other intracellular events, such as increases in ROS and endoplasmic reticulum stress, impair beta cell autophagic activity [5].…”

Section: Introductionmentioning

confidence: 99%

Antibodies to post-translationally modified insulin in type 1 diabetes

et al. 2015

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Aim/hypothesis Insulin is the most specific beta cell antigen and a potential primary autoantigen in type 1 diabetes. Insulin autoantibodies (IAAs) are the earliest marker of beta cell autoimmunity; however, only slightly more than 50% of children and even fewer adults newly diagnosed with type 1 diabetes are IAA positive. The aim of this investigation was to determine if oxidative post-translational modification (oxPTM) of insulin by reactive oxidants associated with islet inflammation generates neoepitopes that stimulate an immune response in individuals with type 1 diabetes. Methods oxPTM of insulin was generated using ribose and various reactive oxygen species. Modifications were analysed by SDS-PAGE, three-dimensional fluorescence and MS. Autoreactivity to oxPTM insulin (oxPTM-INS) was observed by ELISA and western blotting, using sera from participants with type 1 or type 2 diabetes and healthy controls as probes. IAAwas measured using the gold-standard radiobinding assay (RBA). Results MS of oxPTM-INS identified chlorination of Tyr16 and Tyr26; oxidation of His5, Cys7 and Phe24; a nd g l y c at i o n of Lys 2 9 a n d P h e 1 i n ch a i n B . Significantly higher binding to oxPTM-INS vs native insulin was observed in participants with type 1 diabetes, with 84% sensitivity compared with 61% sensitivity for RBA. oxPTM-INS autoantibodies and IAA co-existed in 50% of those with type 1 diabetes. Importantly 34% of those with diabetes who were IAA negative were oxPTM-INS positive. Altogether, 95% of participants with type 1 diabetes presented with autoimmunity to insulin by RBA, oxPTM-INS or both. Binding to oxPTM-INS was directed towards oxPTM-INS fragments with slower mobility than native insulin.

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Section: Introductionmentioning

confidence: 99%

Antibodies to post-translationally modified insulin in type 1 diabetes

et al. 2015

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“…The final stage would be caused by a combination of a deficiency in insulin production and variable insulin sensitivity. In the accompanying For Debate article it is hypothesised that post-translational modification (PTM) of autoantigens might create tissue-specific neo-epitopes that could trigger type 1 diabetes [2]. It should be noted that the contribution by Størling et al [2] truly fulfils the criterion for a 'For Debate' article in that the authors do not provide strong experimental evidence for PTM.…”

mentioning

confidence: 99%

“…In the accompanying For Debate article it is hypothesised that post-translational modification (PTM) of autoantigens might create tissue-specific neo-epitopes that could trigger type 1 diabetes [2]. It should be noted that the contribution by Størling et al [2] truly fulfils the criterion for a 'For Debate' article in that the authors do not provide strong experimental evidence for PTM. Before discussing whether this hypothesis is testable or not, it will first be important to briefly examine the multi-stage character of autoimmune (type 1) diabetes.…”

mentioning

confidence: 99%

“…Størling et al [2] propose that increased expression levels (mRNA, not the enzymes themselves) of enzymes with potential PTM activity after in vitro exposure of human islets to certain cytokines indicates that PTM of autoantigens might take place. Regrettably, there are quite a number of candidate PTM enzymes to sort through.…”

mentioning

confidence: 99%

“…Autoantibodies to IA-2 and ZnT8 were negatively associated with DQ2 [18,19]. A major question not asked by Størling et al is whether the loading of peptides in the binding cleft of the HLA Class II heterodimer is affected by PTMs [2]. Are post-translationally modified peptides loaded at all?…”

mentioning

confidence: 99%

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